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ICOS 受体通过诱导转录抑制因子 Bcl6 来指示 T 滤泡辅助细胞向效应细胞分化。

ICOS receptor instructs T follicular helper cell versus effector cell differentiation via induction of the transcriptional repressor Bcl6.

机构信息

Division of Vaccine Discovery, La Jolla Institute for Allergy and Immunology, La Jolla, CA 92037, USA.

出版信息

Immunity. 2011 Jun 24;34(6):932-46. doi: 10.1016/j.immuni.2011.03.023.

Abstract

The nature of follicular helper CD4(+) T (Tfh) cell differentiation remains controversial, including the minimal signals required for Tfh cell differentiation and the time at which Tfh cell differentiation occurs. Here we determine that Tfh cell development initiates immediately during dendritic cell (DC) priming in vivo. We demonstrate that inducible costimulator (ICOS) provides a critical early signal to induce the transcription factor Bcl6, and Bcl6 then induces CXCR5, the canonical feature of Tfh cells. Strikingly, a bifurcation between Tfh and effector Th cells was measurable by the second cell division of CD4(+) T cells, at day 2 after an acute viral infection: IL2Rα(int) cells expressed Bcl6 and CXCR5 (Tfh cell program), whereas IL2Rα(hi) cells exhibited strong Blimp1 expression that repressed Bcl6 (effector Th cell program). Virtually complete polarization between Bcl6(+) Tfh cells and Blimp1(+) effector Th cell populations developed by 72 hr, even without B cells. Tfh cells were subsequently lost in the absence of B cells, demonstrating a B cell requirement for maintenance of Bcl6 and Tfh cell commitment via sequential ICOS signals.

摘要

滤泡辅助性 CD4(+) T(Tfh)细胞分化的本质仍存在争议,包括 Tfh 细胞分化所需的最小信号以及 Tfh 细胞分化发生的时间。在这里,我们确定 Tfh 细胞的发育在体内树突状细胞(DC)初始激活时立即开始。我们证明诱导共刺激分子(ICOS)提供了一个关键的早期信号,诱导转录因子 Bcl6 的表达,然后 Bcl6 诱导 CXCR5 的表达,这是 Tfh 细胞的典型特征。引人注目的是,在急性病毒感染后第 2 天,CD4(+)T 细胞的第二次细胞分裂时即可测量到 Tfh 和效应 Th 细胞之间的分叉:IL2Rα(int)细胞表达 Bcl6 和 CXCR5(Tfh 细胞程序),而 IL2Rα(hi)细胞则表现出强烈的 Blimp1 表达,抑制 Bcl6(效应 Th 细胞程序)。即使没有 B 细胞,到 72 小时时,Bcl6(+)Tfh 细胞和 Blimp1(+)效应 Th 细胞群之间几乎完全极化,Tfh 细胞随后在没有 B 细胞的情况下消失,这表明 B 细胞通过连续的 ICOS 信号维持 Bcl6 和 Tfh 细胞的定向分化是必需的。

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